Plan of the lecture
Glomerulonephritis (Gn): definition
Epidemiology
Etiology
Pathogenesis
Immuncomplex glomerulonephritis factors
Autoimmune mechanism of glomerulonephritis development differs from immunocomplex process only by its initial steps. Effector process is common due to:
Morphologic forms of glomerulonephritis
Classification of primary glomerulonephritis
Process course activity
Kidney functioning condition
NEPHRITIC SYNDROME
Isolated urine syndrome
NEPHROTIC SYNDROME
Standards of lab testing
Glomerulonephritis treatment
Medications:
Outpatient care
Subacute rapidly progressive (crescentic) GN
Risk factors for CKD development
Glomerular filtration rate
Formula for GFR calculation
Hystologic types of CKD
CKD treatment
Chronic kidney failure
CKD and CKF classification
Chronic kidney failure (CKF) etiology
CKF syndromes and reasons of their development
Diet in CKF
Hemodialysis
Questions
435.50K
Категория: МедицинаМедицина

Glomerulonephritis in children chronic kidney failure

1.

GLOMERULONEPHRITIS in
CHILDREN
CHRONIC KIDNEY FAILURE

2. Plan of the lecture


1. Definition of glomerulonephritis
2. Risk factors and etiology
3. Pathogenesis
4. Classification
5. Diagnostic criteria
• 6. Treatment and prophylaxis

3. Glomerulonephritis (Gn): definition

• Gn is heterogeneous group of
inflammatory immune-complex
diseases predominantly of kidney
glomerular apparatus with different
clinical and morphological
presentation, course and outcome.

4. Epidemiology

• Glomerulonephritis take 3-4 place among
all urinary tract diseases;
• Morbidity is more frequent in 3-12 years
old, but children of all ages can be
affected. If glomerulonephritis occur after
10 years old it is more frequently chronic
form or resistant for steroid therapy.

5. Etiology

• Any diseases that are caused by Streptococcal infections of
group A : 4, 6, 12, 18, 25, 49 strains (like angina, scarlet fever,
piodermia);
• Viral infections (adenoviral, flu, ЕСНО 9, Cocsakie, Varicella,
epidemic parotitis);
• Autoantibodies for mesangeal epithelial, basal, nuclear
antigenes;
• Noninfectious factors: overcooling, repeated vaccinations and
serum medications injections, trauma, insolation, some
medications that release autoantigenes;
• Idiopathic (IgA-nephropathy, membranous-proliferative
glomerulonephritis of I-II types).

6. Pathogenesis

• Main mechanism is immunopathologic
reactions;
• There are 2 main mechanisms:
immunocomplex (in 80-85%) and
autoimmune;

7. Immuncomplex glomerulonephritis factors

• Disturbances of immune complexes clearance from
circulation;
• Compliment system pathology that leads to impairment
of immune complexes inhibition;
• Disturbances of erythrocyte clearance of immune
complexes due to pathology of CR1-receptors in
erythrocytes;
• Functional blockage of mononucleal phagocutes Fcreceptors in liver and spleen;
• Excess of immune complexes formation with peculiar
sizes and charge that capable connect with target
organs and tissues

8. Autoimmune mechanism of glomerulonephritis development differs from immunocomplex process only by its initial steps. Effector process is common due to:

• Presence of common criss-cross antigenes of
microorganisms (bacteria, viruses) and basal
membrane and absence of tolerance;
• Appearance of HLA complexes (DR2 и DR3)on
glomerular basal membrane;
• Kidney tissue damage and releasing of hidden
antigenes or glomerular membranes
dterminants that has no immune tolerance.

9.

The only necessary condition
for glomerulonephritis
development due to
autoimmune mechanism is
specific immunodefficiancy
with decreased function of Tsupressors.

10. Morphologic forms of glomerulonephritis

• Minimal glomerular changes:
increased cellularity, basic
substance, basal membrane
edema, podocyte pedunculy
destruction, but absence of Ig
and fibrinogene deposits like in
nephrotic syndrome
• Focal-segmental
glomerulosclerosis/gyalinosis:
more frquently juksta-glomerular
parts are affected (Berge disease
or Ig-A nephropathy)

11.

• Diffuse Gn (80% and more glomerulus are affected)
– Membranous Gn: diffuse uniform capillary walls
thickening in glomerulars without cell proliferation and
matrix increasing but with thorn development on basal
membrane;
– Diffuse proliferative
– Mesangiocapillary Gn
• Mesangeal proliferative Gn
• Endocapillary proliferative
• Fibroplastic Gn
• Gn with semilunaris (crescentic) (subacute fast
progressive Gn)

12. Classification of primary glomerulonephritis

ACUTE GLOMERULONEPHRITIS:
• Nephritic syndrome;
• Isolated urinary syndrome;
• Nephrotic syndrome;
• Nephrotic with hypertension and
hematuria

13.

CHRONIC GLOMERULONEPHRITIS:
• Hematuric form;
• Nephrotic form;
• Mixed form.
SUBACUTE (MALIGNANT)
GLOMERULONEPHRITIS

14. Process course activity

Acute Gn
• Initial manifestation;
• Swing period (2-4 weeks);
• Period of clinical regression (2-3 months).
Chronic Gn
• Period of exacerbation;
• Period of partial remission;
• Period of complete clinic-laboratory
remission.

15. Kidney functioning condition

Acute Gn
• Without impairment;
• With kidney functioning impairment;
• Acute kidney failure.
Chronic Gn
• Without impairment;
• With kidney functioning impairment;
• Chronic kidney failure.

16. NEPHRITIC SYNDROME

• Morbidity is frequent at 5-12 y old;
• Streptococcal diseases of oral cavity
and skin as a rule precede 2-4 weeks
before Gn onset;
• Onset of Gn is sudden with
intoxication signs like head ache,
malaise, nausea

17.

• Paleness of skin (due to
angiospasm)
• Loin pains ( due to kidney
capsule distention because of
parenchyma edema)
• Moderate edema of face, low
extremeties;

18.

• Cardio-vascular abnormalitiestachycardia;
• Arterial hypertension;
• Oliguria can occur;
• Hematuria
(micro
macrohematuria);
or

19.

• Proteinuria not more than 1-2 g/l per
day;
• Frequently moderate anemia, ESR
elevation, leucocytosis ( if infectious
focus is present) can be present
• Dysproteinemia, ASL”O” more than
250 IU, hyperfibrinogenemia;
• Kidney function insufficiency can be
present

20. Isolated urine syndrome

• Onset is steady without any
subjective symptoms and
extrarenal signs. There are only
urine changes like hematuria,
moderate proteinuria, cylindruria

21. NEPHROTIC SYNDROME

• Typical for preschools (1,5-5 y
old)
• Frequently family history has
allergologic anamnesis;

22.

• Onset is steady with edema
development that can be excessive.
Edema can be peripheral, cavitary,
and very significant like anasarka.
Sudden onset is possible.

23.

• Olyguria
• Significant proteinuria more than 3 g/l per
day.;
• Blood tests – hypoproteinemia predominantly
due to hypoalbuminemia, high hyperlipidemia
and cholesterolemia, hyperfibvrinogenemia;
• ESR is elevated to 50-70 mm/h

24.

NВ !
BP is normal, hematuria isn’t
present, kidney function
failure isn’t typical

25. Standards of lab testing

Obligatory lab studies
– Common blood test +thrombocyte count;
– Biochemical tests (proteinogram, cholesterol,
creatinine, urea etc.);
– Common urine tests;
– Daily diuresis with daily protein loss;
– Nechiporenko test;
– Zimnitsky urine test;
– Immune tests (ASL-O, CIC, IgM, IgA, compliment
system).

26.

Specifying tests (if necessary))
– Blood electrolites ( in stimulated urination,
corticosteroid treatment)
– Liver tests (especially in cytotoxic drugs
treatment)
– Glucose tests (corticosteroid treatment);
– Coagulative tests (desaggrigant,
anticoagulative therapy, DIC -syndrome);
– Daily proteinurea ( in case of protein
losses);
– Creatinine clearance (if kidney function is
impaired);
– Uroleucogram and bacterial culture tests of
urine (if leucocyteurea is present).

27.

Additional lab tests
Of blood
• Antibodies to glomerular basal membrane and neutrophyl cytoplasm
(ANCA);
• Lipidogram;
• Acidic-basic ratio;
• Kidney functioning tests;
• Fibrin products degradation (protaminesulphate and ethanol tests);
• Antinuclear antibodies, LE-cells;
• HLA-typing;
• Markers of hepatite testing;
• Etc..
Urine
• Osmolality testing
• В-2-microglobuline studying
• Lysozyme detection
Throat
• Streptococus smears
• Microscopy of buccal washings
Stool
• Coprogram

28.

Obligatory instrumental testing
Type of testing
Gn stage
Frequency
BP monitoring
Exacerbation
Regression period
Remission period
Every day
2 times/week
If necessary
Body weighing
In edema
Every day
Mac-Klur test
In hidden edema
If necessary
Retina examining
In exacerbation period, while treating by delagyl
Every day
ECG
In exacerbation
In other cases
Every day
If necessary
Ultrasound of kidneys and
UT
Swing period
Regression period
Remission period
Once
Once
If necessary
Ultrasound diagnostics of
inner organs
Swing period
In other cases
Every day
If necessary
X-ray of bones, lungs
-
If necessary
Radionuclide examining
Swing period
In other cases
Twice
Once per 1-2 years
Punction kidney biopsy
Before treatment
After treatment
Before finishing outpatient care
Once
Once
Once

29. Glomerulonephritis treatment

Regimen is strictly bed type
only if extrarenal symptoms
are present like edema,
hypertension, olygouria,
macrohematuria

30.

–Diet
Is dependant on edema arterial
hypertension
and
functional
kidney capacity. During acute
period salt (NaCl) must be
excluded,
fluids
and
animal
proteins must be restricted. All
these demands are taken into
account in diet N7 (Pevzner)

31. Medications:

• а) etiologic (if infection as initializing
factor is proved or chronic focus of
infection is present-antibiotic treatment
(preferably penicillines);

32.

• b) pathogenic (the main goal is
to eradicate antigen from
organism and supress antibody
production)
• Plasmopheresis or hemasorbtion
(if creatinine, urea level,
hyperfibrinogenemia and
circulated immune complexes
(CIC) are increased

33.

• disaggregants (curantil, ticlid) for 3-4
weeks 2-5 mg/kg per day, than 1/2 of this
dosage for 1-3 month;
• anticoagulants (heparin
50-150 IU/kg 4
times per day with blood coagulation tests
control (Lee-White test);

34.

• Corticosteroids 1,5-2mg/kg per day,
prednisolon for 8 weeks than cyclic
treatment with 1/2 of initial dosage
with steady decreasing of it for 2,5-5
mg once per 1,5 - 2 month;
• Cytostatics (leukeran 0,2 mg/kg per
day for 6-8 weeks, than 1/2 of initial
dosage for 6-8 months).

35.

• Antihypertension, antiproteinuric,
antisclerotic drugs :
• Angitensin converting enzyme
inhibitors (ACEI) –enalapril, lysinopril
– 5-40 mg/day; Angiotensin receptor
blockers (ARB) - (candesar,
telmisartan)
• Ca channel blockers- diltiazem
• в) syndrome therapy: diuretics
(trifas,lasycs,hypothiazid,verospironi
).

36. Outpatient care

• After acute
glomerulonephritis clinicallaboratory remision children
must be for 5 years under
outpatient medical care

37. Subacute rapidly progressive (crescentic) GN

• Crescentic GN is severe form of glomeruli
injury with presence of large crescents in
50% and more glomeruli. The condition
presents with severe acute GN with
azotemia that fails to resolve. It can occur
in poststreptococcal GN or features of
nephrotic syndrome.The long-term
outcome dependsof therapy efficiacy and
its promptness.

38.

Chronic kidney diseases
From 2003 concept “Chronic kidney disease” was introduced to
children nephrology
Criteria of CKD:
1. Lesion of kidneys more than 3 months with structural or
functional features with or without glomerular filtration rate
decreasing and manifested by one or several symptoms listed
below:
• Urine test or blood test changes;
• Visualizing changes during special examinings;
• Biopsy changes.
2. Glomerular filtration rate less than 60 ml/min or 1,73 м2 for 3
months with or without other kidney damages.

39.

• CKD can be independent diagnose or
summerized one;
Like:
• CKD
• CKD: chronic glomerulonephritis,
hematuric form, clinic-lab remission
period.
• Diagnosting of CKD is performed
independently to causative disease.
In this situation we suppose further process
progression even without glomerular
filtration rate decreasing

40. Risk factors for CKD development

• CKD induced factors
Diabetes mellitus 1, 2 type;
Arterial hypertension;
Autoimmune diseases;
Urinary tract infection;
Nephrocalcinosis;
Toxic medication influences.

41.

• Factors induced CKD progression
• High level of proteinurea or arterial
hypertension;
• Insufficient glycemia level control;
• Smoking.
• Risk factors of CKD end-point
• Low dialyze access;
• Temporary vessel access;
• Anemia;
• Low level of albumin;
• Late dialyze treatment.

42. Glomerular filtration rate

• GFR less than 60 ml/min – can be developed
due to CKF without clinical- lab symptoms of
kidney disease.
• GFR less than 60 ml/min means that more
than 50% of nephrones has been destroyed,
but creatinine level can be in the highest
normal level.

43. Formula for GFR calculation

After author of formula
(quantity of studied patients)
Schwartz other
(n=186)
Formula with usage of serum creatinine level and
height
[ 0,0484 * height(sm)]
CCr (ml/min/1,73m2) = -----------------------Scr(mMol/l)
For boys more than 13 years old substitute
coefficient 0,0484 for 0,0616
[ 0,043 * height(sm)]
Konegen and other.
CcR*(ml/min/1,73м2)= ---------------------(n=108)
Scr(mg/dl)
Ссr – creatinine clearance, Scr – serum creatinine.
* - in online regimen calculations of GFR according Schwartz formua is
accessible in Internet: www.nephrology.kiev.ua

44. Hystologic types of CKD

• Proliferative GN ( mesangial
prolifirative GN, crescentic GN,
membranoproliferative GN)
• Focal segmental glomerulosclerosis
• Membranous nephropathy with diffuse
thickening of glomerular basement
membrane

45. CKD treatment

• There is no specific treatment for
chronic GN.
• Steroids and immunosuppressive
drugs can only retard development of
renal sclerosis and progression to
chronic renal failure

46. Chronic kidney failure

is stable irreversible progressive kidney
function disorder due to different
diseases manifested by endogene
createnine clearence decreasing more
than 20ml/min 1,73 m, serum createnine
more than 0,177 mmol/sec, urea more
than 5,8 mmol/l
(4 European Congress of pediatritiansnephrologists Recommendations, Dublin,
1971)

47. CKD and CKF classification

CKD
stage
CKF stage
GFR
мл/мин/1,
73 м2
Blood
creatinine,
mMols/l
Max urine
spec.
gravity
I
-
≥90
≤0,104
›1,018
II
I (tubular)
I (compensated)
≥90
89-60
≤0,104
0,105-0,176
≤1,018
‹1,018
III
II (subcompensated)
59-30
0,177-0,351
‹1,018
IV
III (decompensated)
20-15
0,352-0,440
-
V
IV (terminal /dialyzed )
‹15
›0,440
-

48.

2.Total kidney failure
Serum createnine content 0,17 –0,44 mmols/l:
Glomerulopathies: Hypertension, hemorrhagic
syndrome, acidosis, decreasing of glomerular
filtration rate and tubular functions
Tubulapathies: osteopathies, anemia, acidosis,
glomerular filtration rate and tubular function
limitation
Serum createnine level is 0,44-0,88 mmol/l in first
group disturbancies of inner organ functioning, in
tubulopathies both inner organs functioning and
hemorrhagic syndrome will be present
If createnine concentration is more than 0,88 mmoll/l
symptoms of uremia will be present. This is End
Stage Renal Disease, olygoanuric stage

49. Chronic kidney failure (CKF) etiology

– Glomerulopathies: Primary glomerular dieases,
immuneglobuline A nephropathies, membraneproliferative glomerulonephritis
– Glomerulopathies associated with systemic
diseases – diabetus mellitus, amyloidosis, SLE,
hemolytic-uremic syndrome
– Tubularinterstitial disease:refluxnepohropathies with pyelonephritris,
sarcoidosis, toxic nephropathies
– Inherited diseases: cystic, Alport syndrome
– Hypertension
– Kidney vascular disesases
– Obstructive uropathies

50. CKF syndromes and reasons of their development


CKF syndromes and reasons of their development
Failure to growth and development – hypostature,
malnutrition, sexual development retardation due
to kidney dysembryogenesis, nephrosclerosis,
protein and vitamin defficiency, azotemia, acidosis
Uremia - astenia, anorexia, psychoneurologic
disorders, gastroentherocolitis, pericarditis due to
retention of nitrogenic metabolites and impaired
filtration, enhanced catabolism
Water and electrolite balance disorder –edema,
hyperkaliemia, hypocalciemia, hyponatriemia due
to glomerulo-tubular dysbalance and impaired
electrolyte transport
Metabolic acidosis - nausea, vomiting, dyspnea
due to impaired ammonia- acid filtration,
exhausting buffer reserve

51.

• Arterial hypertension - head ache, hypertonic
crises, retinopathy due to enhanced Pg
production and water –electrolyte dysbalance
• Osteodystrophy – pains in bones, X-ray and
morphologic changes due to impaired VitD
metabolites synthesis and
hyperparathyroidism
• DIC syndrome – Hemorrhagic lesions in
different organs and tissues due to impaired
thrombus formation, rheology, coagulative
disorders
• Immune-deficience –frequent viral and
bacterial infections, septic complications due
to protein deficiency, hormonal dysbalance

52. Diet in CKF

• Diet N 7 : moderate limitation in protein, salt
(not more than 0,4 g/day). Restrict meat, fish,
cottage cheese
• May eat potato, oils, eggs, sour-cream, bread,
pasta
• Day quantity of proteins 0,6 до 1,7 mg/kg per
day
In 3-4 grade of CKF protein intake mustn’t exceed
- 0.5 g/kg per day
• Essential amino-acids can be used as food
additives (ketosteril – 1 trabl/kg per day)

53. Hemodialysis

• Indications:
Glomeruli filtration rate less than10
ml/(min for 1,73sq.м), createnine
more than 0,7 mmols/l , hyperkalemia
more 6,5 mmol/l, «noncontrolled»
hypertension, uremic pericarditis
• Cointraindications:
Multiple malformations, malignancy,
law birth weight, tuberculosis,
hepatitis, GI ulceration parents
refusal

54.

• Indications for kidney
transplantation terminal kidney
failure stage
• Contraindications : mental
diseases, malignancies, sepsis,
chronic purulent lung diseases,
systemic vasculitius, refluxnephropathy, ulcer stomach
diseases, polyserositis, severe
uncontrolled hypertension

55. Questions

• Glomerulonephritis and chronic kidney failure.
• Classification glomerulonephritis and kidney
failure in children.
• What causes glomerulonephritis?
• What causes acute and chronic kidney failure?
• Clinical forms glomerulonephritis.
• Clinical manifestations. Diagnosis.
• Can medicine treat glomerulonephritis?
• Rational antibiotic and hormone treatment.
• Transplantation of kidney.
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